Ciencias,UNAM

Formation of the steroidal 3 beta-hydroxy-6-oxo-moiety. Synthesis and cytotoxicity of glucolaxogenin

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dc.contributor.author Fernandez-Herrera, MA
dc.contributor.author Sandoval-Ramirez, J
dc.contributor.author Sánchez-Sánchez, L
dc.contributor.author López-Muñoz, H
dc.date.accessioned 2011-01-21T10:35:24Z
dc.date.available 2011-01-21T10:35:24Z
dc.date.issued 2009
dc.identifier.issn 1551-7004
dc.identifier.uri http://hdlhandlenet/123456789/217
dc.description.abstract An efficient alternative route to the synthesis of the steroidal 3 beta-hydroxy-6-oxo moiety starting from diosgenin and cholesterol is described. The sequential tosylation, oxidative hydroboration, and selective reduction steps provided the target 3 beta-hydroxy-6-oxo moiety, yielding laxogenin 1 in 82% and 3 beta-hydroxycholestan-6-one 8 in 83% overall yield. The cleavage of the S-O bond of 3 beta-tosylate-6-oxo intermediates was succeeded by means of sodium naphthalenide at -80 degrees C en_US
dc.description.abstract when the reduction was explored at room temperature the cleavage of the C-O bond was favored and the corresponding i-steroids were observed. Glucolaxogenin 15 was synthesized in 68% from 1, and its antiproliferative activity was evaluated in cervical cancer cells HeLa, CaSki and ViBo. The effect on peripheral blood lymphocytes was assessed founding that the cell growth was unaffected showing therefore high selectivity. en_US
dc.language.iso en en_US
dc.title Formation of the steroidal 3 beta-hydroxy-6-oxo-moiety. Synthesis and cytotoxicity of glucolaxogenin en_US
dc.type Article en_US
dc.identifier.idprometeo 63
dc.source.novolpages :170-184
dc.subject.wos Chemistry, Organic
dc.description.index WoS: SCI, SSCI o AHCI
dc.subject.keywords 3 beta-Hydroxy-6-oxo moiety
dc.subject.keywords sodium naphthalenide
dc.subject.keywords cervical cancer cells
dc.subject.keywords glucolaxogenin
dc.subject.keywords lymphocytes
dc.relation.journal Arkivoc

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